Abe T, Sugaya H, Ishida K, Khan W I, Tasdemir I, Yoshimura K
Department of Parasitology, Akita University School of Medicine, Japan.
Immunology. 1993 Sep;80(1):116-21.
Information about interleukin-3 (IL-3) effects in vivo is limited compared with the in vitro effects. We found that a repetitive injection of a low dose of recombinant IL-3 induced protection against intestinal worms of Strongyloides ratti in C57BL/6 mice. When mice were injected i.p. with different doses of recombinant IL-3 twice a day from day -5 to day -1 and infected orally with larvae recovered from the head of infected rats on day 0, worm recovery from the small intestine was markedly reduced by a total of 10(4) U IL-3 or more on day 2 post-infection. The number of intestinal mucosal mast cells (MMC) was increased by the protective dose of IL-3. The IL-3 treatment, however, was ineffective in protecting mice against tissue migrating larvae, as assessed by recovery from the head. The protective effect of IL-3 on intestinal worms was observed within 6 hr post oral infection, suggesting little concern with antigen-specific immune responses. The effective dose of IL-3 treatment increased the number of MMC progenitors five times in the spleen and the mesenteric lymph nodes. An MMC-specific protease, MMCP-1, was secreted 200 times more than in controls in the intestinal lumen by the IL-3 treatment. The IL-3 treatment induced no protection or mastocytosis in mast cell-deficient W/Wv mice. These results suggest that the IL-3-induced intestinal protection against S. ratti is mediated by MMC.
与白细胞介素-3(IL-3)的体外作用相比,其体内作用的相关信息有限。我们发现,重复注射低剂量重组IL-3可诱导C57BL/6小鼠对鼠类圆线虫肠道蠕虫产生保护作用。从第-5天至第-1天,每天给小鼠腹腔注射不同剂量的重组IL-3两次,并于第0天经口感染从感染大鼠头部获取的幼虫,在感染后第2天,总共10(4) U或更多的IL-3可显著减少从小肠中回收的蠕虫数量。肠道黏膜肥大细胞(MMC)的数量因IL-3的保护剂量而增加。然而,通过从头部回收情况评估,IL-3治疗对保护小鼠免受组织迁移幼虫的侵害无效。在经口感染后6小时内观察到IL-3对肠道蠕虫的保护作用,这表明对抗原特异性免疫反应的影响较小。IL-3治疗的有效剂量使脾脏和肠系膜淋巴结中的MMC祖细胞数量增加了五倍。IL-3治疗使肠腔内MMC特异性蛋白酶MMCP-1的分泌量比对照组多200倍。IL-3治疗在肥大细胞缺陷的W/Wv小鼠中未诱导出保护作用或肥大细胞增多症。这些结果表明,IL-3诱导的对鼠类圆线虫的肠道保护作用是由MMC介导的。
